Baicalein, an active component of Scutellaria baicalensis Georgi, prevents lysophosphatidylcholine-induced cardiac injury by reducing reactive oxygen species production, calcium overload and apoptosis via MAPK pathways

Lysophosphatidylcholine (lysoPC) is generated by the phospholipase A2-dependent hydrolysis of phosphatidylcholine in the membranes of injured cardiomyocytes and may cause deleterious effects on cardiac function during cardiac ischemia [1]. In addition, lysoPC can induce the increase of the intracellular Ca²⁺ concentration ([Ca²⁺]i) and plays an important role in triggering onset of arrhythmias in cardiac ischemia [2]. Besides, lysoPC triggers apoptosis of vascular smooth muscle cells and endothelial cells by altering intracellular calcium signaling [3, 4]. LysoPC also is one of the key components accumulating in the atherosclerotic lesions, and participate in the initiation and/or progression of atherosclerosis [3‐5].

Oxidative stress in cardiomyocytes plays an important role in the pathogenesis of both heart failure and ischemic reperfusion injury. The reactive oxygen species (ROS) can cause severe myocardium damage because the cardiac system carries lesser superoxide dismutase, glutathione, and catalase to remove the superoxidative toxic substances [6]. Huang Qui (Scutellaria baicalensis Gerorgi) is a raw material of traditional Chinese Pharmacopoeia commonly used to improve the physique, and resist inflammation and microorganisms. The compositions of baicalein, wagonin, skullcap-flavone I & II in Huang Qui all have anti-oxidative effects, so Huang Qui has been implicated in the prevention of the ischemia-reperfusion injuries and in the reduction of the ROS productions [7, 8]. Baicalein (5,6,7-trihydroxy-2-phenyl-4H-1-benzopyran-4-one) is a major bioactive flavones constituent of Huang Qui, and shows a variety of biological activities, including antioxidant, anti-inflammatory, antithrombotic, antiviral, and anticancer activities. In deed, in previous studies baicalein has been found to effectively lower ROS-induced cells death in chicken fetal cardiomyocytes in the setting of hypoxic injury [7‐9].

Baicalein has previously been shown to possess not only anti-apoptotic effects on cardiomyocytes but also anti-proliferative effects in VSMCs [7‐9]. However, it is unclear whether this agent may protect cardiomyocytes from lysoPC-induced cytotoxicity, and if so, what the underlying mechanisms are. Therefore, this study was undertaken to determine the protective effects and mechanisms of baicalein in lysoPC-induced cytotoxicity in H9c2 cardiomyocytes.

It has been reported that the concentration of lysoPC in myocardium may increase in the setting of cardiac ischemia [12, 13]. In addition, it is known that lysoPC could cause the Ca²⁺-influx in rat cardiomyocytes [14]. LysoPC accumulation in intracellular and/or interstitial space in cardiomyocytes may underlie as a mechanism for tachycardia and various arrhythmias during cardiac ischemia, which is usually accompanied by elevation of [Ca²⁺]i [2]. The exogenous lysoPC was also proven to induce myoischemia-like injury in in vitro study. As the increase of [Ca²⁺]i would cause irreversible injury of cardiomyocytes including reduction of cell-to-cell coupling, abnormal rhythmic activity and malignant intra-cardiac reentry, preservation of the level of [Ca²⁺]i within normal range is important for the normalization of cardiac function [2, 13‐15]. Therefore, a drug that can minimize the detrimental effects of lysoPC could attenuate cardiac dysfunction during myocardial ischemia. Here we show that baicalein attenuated cell death, apoptosis, and [Ca²⁺]i accumulation of H9c2 cells caused by lysoPC in a dose-dependent manner. Our results are in line with recent investigations showing that baicalein protects against balloon injury-induced intimal hyperplasia and aortic banding-induced cardiac hypertrophy and fibrosis [16, 17]. Therefore, baicalein might have the therapeutic utility in the treatment of cardiovascular disease.

Overproduction of ROS may lead to cell death and apoptosis [6]. Recently studies strengthen the notion that ROS is an important mediator of lysoPC-induced cytotoxicity in both endothelial cells and VSMCs. Previous study suggested that ROS generated through NADH/NADPH oxidase are essential for the growth-promoting signals activated by lysoPC in VSMCs [18]. Oxidative stress promotes the apoptosis or death of cardiomyocytes and has been implicated in cardiovascular diseases, and the Bcl-2 family proteins are known as key regulators of the apoptotic response [19, 20]. In present study, pretreatment of baicalein induced up-regulated the expression of Bcl-2 protein and down-regulated the production of Bax protein in H9c2 cells, resulting in a dramatic decrease in the Bax to Bcl-2 ratio, and also blocked the release of cytochrome c and activation of caspase-3 and caspase-9. The mechanisms of anti-apoptotic effects of Bcl-2 include: (1) act against the apoptotic gene of Bax; (2) inhibit the secretion of cytochrome c from the mitochondria to the cytoplasma, which are promoters of apoptosis; (3) block the trigger effects of cytochrome C on caspase cascades; and (4) induce the Bcl-2 proteins to carry the effects of anti-oxidation and stabilize the level of intracellular Ca²⁺. Actually, the ratio between the Bcl-2 and Bax helps to determine the susceptibility of cells to a death signal, and it has been suggested that the Bcl-2/Bax ratio may be more important than either promoter alone, in determining the apoptosis pathway [19‐21].

MAPK family, one of downstream signal transduction pathways of ROS, is believed to function as integrators for cell growth, survival and apoptosis. In general, the p38 cascade mediates the apoptosis and the reactions of cytokines; the JNK cascade mediates inflammation, cell differentiation, and apoptosis; and the ERK cascade regulates cell differentiation and growth [22, 23]. It is generally believed that phosphorylation of ERK1/2 can protect apoptosis of cardiomyocytes. However, there is some evidence suggesting that ERK1/2 also contributes to cell death of cardiomyocytes. For example, activation of ERK1/2 has a role in Bcl-2 family-mediated cell apoptosis caused by doxorubicin in cardiomyocytes [24]. In our study baicalein inhibited activations of all three MAPK induced by lysoPC, we speculate that the effect on ERK was offset by those beneficial effects on JNK and p38, resulting in net effects of preserving cell survival.

The protective effects of baicalein are summarized and shown in Figure 8. In the study, we found baicalein not only inhibited the lysoPC-induced ROS production and intracellular Ca²⁺ accumulation, but also inhibited the three families of MAPK kinases (p38, JNK, and ERK) as well as the mitochondrial intrinsic apoptotic pathway.

There are two limitations of this study. First, the H9c2 cardiomyoblasts instead of cardiomyocytes were used in our study. The H9c2 cell line was derived from the embryonic rat heart, presenting similar properties of cardiomyocytes. However, future studies may be warranted to substantiate these findings in cardiomyocytes and myocardial tissue. Second, we decreased the highest dose of lysoPC from 50 μM to 10 μM in some experiments (MAPK and apoptosis). The reason is that high concentration of lysoPC (50 μM) could decrease of cell viability significantly, so that it was difficult to collect enough viable cells to perform these analysis.

In summary, these novel results indicate that baicalein can protect H9c2 cells from lysoPC-induced cell death via reducing ROS production and anti-apoptosis. Such protective effects are possibly mediated through reduction of calcium overload, the mitochondrial intrinsic apoptotic pathway, and the MAPK signaling pathway. Thus, this study provides a cellular and molecular basis for baicalein in the treatment of lysoPC-induced cardiac injury.